Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers

Background: Most of the patients with Pancreatic Ductal Adenocarcinoma (PDA) are not eligible for a curative surgical resection. For this reason there is an urgent need for personalized therapies. PDA is the result of complex interactions between tumor molecular profile and metabolites produced by i...

Descripción completa

Detalles Bibliográficos
Autores principales: Follia, Laura, Ferrero, Giulio, Mandili, Giorgia, Beccuti, Marco, Giordano, Daniele, Spadi, Rosella, Satolli, Maria Antonietta, Evangelista, Andrea, Katayama, Hiroyuki, Hong, Wang, Momin, Amin A., Capello, Michela, Hanash, Samir M., Novelli, Francesco, Cordero, Francesca
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6400843/
https://www.ncbi.nlm.nih.gov/pubmed/30873387
http://dx.doi.org/10.3389/fonc.2019.00115
_version_ 1783400030430822400
author Follia, Laura
Ferrero, Giulio
Mandili, Giorgia
Beccuti, Marco
Giordano, Daniele
Spadi, Rosella
Satolli, Maria Antonietta
Evangelista, Andrea
Katayama, Hiroyuki
Hong, Wang
Momin, Amin A.
Capello, Michela
Hanash, Samir M.
Novelli, Francesco
Cordero, Francesca
author_facet Follia, Laura
Ferrero, Giulio
Mandili, Giorgia
Beccuti, Marco
Giordano, Daniele
Spadi, Rosella
Satolli, Maria Antonietta
Evangelista, Andrea
Katayama, Hiroyuki
Hong, Wang
Momin, Amin A.
Capello, Michela
Hanash, Samir M.
Novelli, Francesco
Cordero, Francesca
author_sort Follia, Laura
collection PubMed
description Background: Most of the patients with Pancreatic Ductal Adenocarcinoma (PDA) are not eligible for a curative surgical resection. For this reason there is an urgent need for personalized therapies. PDA is the result of complex interactions between tumor molecular profile and metabolites produced by its microenvironment. Despite recent studies identified PDA molecular subtypes, its metabolic classification is still lacking. Methods: We applied an integrative analysis on transcriptomic and genomic data of glycolytic genes in PDA. Data were collected from public datasets and molecular glycolytic subtypes were defined using hierarchical clustering. The grade of purity of the cancer samples was assessed estimating the different amount of stromal and immunological infiltrate among the identified PDA subtypes. Analyses of metabolomic data from a subset of PDA cell lines allowed us to identify the different metabolites produced by the metabolic subtypes. Sera of a cohort of 31 PDA patients were analyzed using Q-TOF mass spectrometer to measure the amount of metabolic circulating proteins present before and after chemotherapy. Results: Our integrative analysis of glycolytic genes identified two glycolytic and two non-glycolytic metabolic PDA subtypes. Glycolytic patients develop disease earlier, have poor prognosis, low immune-infiltrated tumors, and are characterized by a gain in chr12p13 genomic region. This gain results in the over-expression of GAPDH, TPI1, and FOXM1. PDA cell lines with the gain of chr12p13 are characterized by an higher lipid uptake and sensitivity to drug targeting the fatty acid metabolism. Our sera proteomic analysis confirms that TPI1 serum levels increase in poor prognosis gemcitabine-treated patients. Conclusions: We identify four metabolic PDA subtypes with different prognosis outcomes which may have pivotal role in setting personalized treatments. Moreover, our data suggest TPI1 as putative prognostic PDA biomarker.
format Online
Article
Text
id pubmed-6400843
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-64008432019-03-14 Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers Follia, Laura Ferrero, Giulio Mandili, Giorgia Beccuti, Marco Giordano, Daniele Spadi, Rosella Satolli, Maria Antonietta Evangelista, Andrea Katayama, Hiroyuki Hong, Wang Momin, Amin A. Capello, Michela Hanash, Samir M. Novelli, Francesco Cordero, Francesca Front Oncol Oncology Background: Most of the patients with Pancreatic Ductal Adenocarcinoma (PDA) are not eligible for a curative surgical resection. For this reason there is an urgent need for personalized therapies. PDA is the result of complex interactions between tumor molecular profile and metabolites produced by its microenvironment. Despite recent studies identified PDA molecular subtypes, its metabolic classification is still lacking. Methods: We applied an integrative analysis on transcriptomic and genomic data of glycolytic genes in PDA. Data were collected from public datasets and molecular glycolytic subtypes were defined using hierarchical clustering. The grade of purity of the cancer samples was assessed estimating the different amount of stromal and immunological infiltrate among the identified PDA subtypes. Analyses of metabolomic data from a subset of PDA cell lines allowed us to identify the different metabolites produced by the metabolic subtypes. Sera of a cohort of 31 PDA patients were analyzed using Q-TOF mass spectrometer to measure the amount of metabolic circulating proteins present before and after chemotherapy. Results: Our integrative analysis of glycolytic genes identified two glycolytic and two non-glycolytic metabolic PDA subtypes. Glycolytic patients develop disease earlier, have poor prognosis, low immune-infiltrated tumors, and are characterized by a gain in chr12p13 genomic region. This gain results in the over-expression of GAPDH, TPI1, and FOXM1. PDA cell lines with the gain of chr12p13 are characterized by an higher lipid uptake and sensitivity to drug targeting the fatty acid metabolism. Our sera proteomic analysis confirms that TPI1 serum levels increase in poor prognosis gemcitabine-treated patients. Conclusions: We identify four metabolic PDA subtypes with different prognosis outcomes which may have pivotal role in setting personalized treatments. Moreover, our data suggest TPI1 as putative prognostic PDA biomarker. Frontiers Media S.A. 2019-02-27 /pmc/articles/PMC6400843/ /pubmed/30873387 http://dx.doi.org/10.3389/fonc.2019.00115 Text en Copyright © 2019 Follia, Ferrero, Mandili, Beccuti, Giordano, Spadi, Satolli, Evangelista, Katayama, Hong, Momin, Capello, Hanash, Novelli and Cordero. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Follia, Laura
Ferrero, Giulio
Mandili, Giorgia
Beccuti, Marco
Giordano, Daniele
Spadi, Rosella
Satolli, Maria Antonietta
Evangelista, Andrea
Katayama, Hiroyuki
Hong, Wang
Momin, Amin A.
Capello, Michela
Hanash, Samir M.
Novelli, Francesco
Cordero, Francesca
Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers
title Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers
title_full Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers
title_fullStr Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers
title_full_unstemmed Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers
title_short Integrative Analysis of Novel Metabolic Subtypes in Pancreatic Cancer Fosters New Prognostic Biomarkers
title_sort integrative analysis of novel metabolic subtypes in pancreatic cancer fosters new prognostic biomarkers
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6400843/
https://www.ncbi.nlm.nih.gov/pubmed/30873387
http://dx.doi.org/10.3389/fonc.2019.00115
work_keys_str_mv AT follialaura integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT ferrerogiulio integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT mandiligiorgia integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT beccutimarco integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT giordanodaniele integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT spadirosella integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT satollimariaantonietta integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT evangelistaandrea integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT katayamahiroyuki integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT hongwang integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT mominamina integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT capellomichela integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT hanashsamirm integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT novellifrancesco integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers
AT corderofrancesca integrativeanalysisofnovelmetabolicsubtypesinpancreaticcancerfostersnewprognosticbiomarkers

Ejemplares similares